Medicine (Austin & Northern Health) - Research Publications

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Author: Bellows, Susannah × Author: Scheffer, Ingrid × End date: 2014 ×

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    Dravet syndrome as epileptic encephalopathy: evidence from long-term course and neuropathology
    Catarino, CB ; Liu, JYW ; Liagkouras, I ; Gibbons, VS ; Labrum, RW ; Ellis, R ; Woodward, C ; Davis, MB ; Smith, SJ ; Cross, JH ; Appleton, RE ; Yendle, SC ; McMahon, JM ; Bellows, ST ; Jacques, TS ; Zuberi, SM ; Koepp, MJ ; Martinian, L ; Scheffer, IE ; Thom, M ; Sisodiya, SM (OXFORD UNIV PRESS, 2011-10)
    Dravet syndrome is an epilepsy syndrome of infantile onset, frequently caused by SCN1A mutations or deletions. Its prevalence, long-term evolution in adults and neuropathology are not well known. We identified a series of 22 adult patients, including three adult post-mortem cases with Dravet syndrome. For all patients, we reviewed the clinical history, seizure types and frequency, antiepileptic drugs, cognitive, social and functional outcome and results of investigations. A systematic neuropathology study was performed, with post-mortem material from three adult cases with Dravet syndrome, in comparison with controls and a range of relevant paediatric tissue. Twenty-two adults with Dravet syndrome, 10 female, were included, median age 39 years (range 20-66). SCN1A structural variation was found in 60% of the adult Dravet patients tested, including one post-mortem case with DNA extracted from brain tissue. Novel mutations were described for 11 adult patients; one patient had three SCN1A mutations. Features of Dravet syndrome in adulthood include multiple seizure types despite polytherapy, and age-dependent evolution in seizure semiology and electroencephalographic pattern. Fever sensitivity persisted through adulthood in 11 cases. Neurological decline occurred in adulthood with cognitive and motor deterioration. Dysphagia may develop in or after the fourth decade of life, leading to significant morbidity, or death. The correct diagnosis at an older age made an impact at several levels. Treatment changes improved seizure control even after years of drug resistance in all three cases with sufficient follow-up after drug changes were instituted; better control led to significant improvement in cognitive performance and quality of life in adulthood in two cases. There was no histopathological hallmark feature of Dravet syndrome in this series. Strikingly, there was remarkable preservation of neurons and interneurons in the neocortex and hippocampi of Dravet adult post-mortem cases. Our study provides evidence that Dravet syndrome is at least in part an epileptic encephalopathy.
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    Does variation in NIPA2 contribute to genetic generalized epilepsy?
    Hildebrand, MS ; Damiano, JA ; Mullen, SA ; Bellows, ST ; Scheffer, IE ; Berkovic, SF (SPRINGER, 2014-05)
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    Glucose metabolism transporters and epilepsy: Only GLUT1 has an established role
    Hildebrand, MS ; Damiano, JA ; Mullen, SA ; Bellows, ST ; Oliver, KL ; Dahl, H-HM ; Scheffer, IE ; Berkovic, SF (WILEY, 2014-02)
    The availability of glucose, and its glycolytic product lactate, for cerebral energy metabolism is regulated by specific brain transporters. Inadequate energy delivery leads to neurologic impairment. Haploinsufficiency of the glucose transporter GLUT1 causes a characteristic early onset encephalopathy, and has recently emerged as an important cause of a variety of childhood or later-onset generalized epilepsies and paroxysmal exercise-induced dyskinesia. We explored whether mutations in the genes encoding the other major glucose (GLUT3) or lactate (MCT1/2/3/4) transporters involved in cerebral energy metabolism also cause generalized epilepsies. A cohort of 119 cases with myoclonic astatic epilepsy or early onset absence epilepsy was screened for nucleotide variants in these five candidate genes. No epilepsy-causing mutations were identified, indicating that of the major energetic fuel transporters in the brain, only GLUT1 is clearly associated with generalized epilepsy.
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    Seizure semiology in autosomal dominant epilepsy with auditory features, due to novel LGI1 mutations
    Sadleir, LG ; Agher, D ; Chabrol, E ; Elkouby, L ; Leguern, E ; Paterson, SJ ; Harty, R ; Bellows, ST ; Berkovic, SF ; Scheffer, IE ; Baulac, S (ELSEVIER SCIENCE BV, 2013-12)
    Mutations in LGI1 are found in 50% of families with autosomal dominant epilepsy with auditory features (ADEAF). In ADEAF, family members have predominantly lateral temporal lobe seizures but mesial temporal lobe semiology may also occur. We report here three families with novel LGI1 mutations (p.Ile82Thr, p.Glu225*, c.432-2_436del). Seven affected individuals reported an auditory aura and one a visual aura. A 10-year old boy described a cephalic aura followed by an unpleasant taste and oral automatisms without auditory, visual or psychic features.
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    Genome-wide association analysis of genetic generalized epilepsies implicates susceptibility loci at 1q43, 2p16.1, 2q22.3 and 17q21.32
    Steffens, M ; Leu, C ; Ruppert, A-K ; Zara, F ; Striano, P ; Robbiano, A ; Capovilla, G ; Tinuper, P ; Gambardella, A ; Bianchi, A ; La Neve, A ; Crichiutti, G ; de Kovel, CGF ; Trenite, DK-N ; de Haan, G-J ; Lindhout, D ; Gaus, V ; Schmitz, B ; Janz, D ; Weber, YG ; Becker, F ; Lerche, H ; Steinhoff, BJ ; Kleefuss-Lie, AA ; Kunz, WS ; Surges, R ; Elger, CE ; Muhle, H ; von Spiczak, S ; Ostertag, P ; Helbig, I ; Stephani, U ; Moller, RS ; Hjalgrim, H ; Dibbens, LM ; Bellows, S ; Oliver, K ; Mullen, S ; Scheffer, IE ; Berkovic, SF ; Everett, KV ; Gardiner, MR ; Marini, C ; Guerrini, R ; Lehesjoki, A-E ; Siren, A ; Guipponi, M ; Malafosse, A ; Thomas, P ; Nabbout, R ; Baulac, S ; Leguern, E ; Guerrero, R ; Serratosa, JM ; Reif, PS ; Rosenow, F ; Moerzinger, M ; Feucht, M ; Zimprich, F ; Kapser, C ; Schankin, CJ ; Suls, A ; Smets, K ; De Jonghe, P ; Jordanova, A ; Caglayan, H ; Yapici, Z ; Yalcin, DA ; Baykan, B ; Bebek, N ; Ozbek, U ; Gieger, C ; Wichmann, H-E ; Balschun, T ; Ellinghaus, D ; Franke, A ; Meesters, C ; Becker, T ; Wienker, TF ; Hempelmann, A ; Schulz, H ; Rueschendorf, F ; Leber, M ; Pauck, SM ; Trucks, H ; Toliat, MR ; Nuernberg, P ; Avanzini, G ; Koeleman, BPC ; Sander, T (OXFORD UNIV PRESS, 2012-12-15)
    Genetic generalized epilepsies (GGEs) have a lifetime prevalence of 0.3% and account for 20-30% of all epilepsies. Despite their high heritability of 80%, the genetic factors predisposing to GGEs remain elusive. To identify susceptibility variants shared across common GGE syndromes, we carried out a two-stage genome-wide association study (GWAS) including 3020 patients with GGEs and 3954 controls of European ancestry. To dissect out syndrome-related variants, we also explored two distinct GGE subgroups comprising 1434 patients with genetic absence epilepsies (GAEs) and 1134 patients with juvenile myoclonic epilepsy (JME). Joint Stage-1 and 2 analyses revealed genome-wide significant associations for GGEs at 2p16.1 (rs13026414, P(meta) = 2.5 × 10(-9), OR[T] = 0.81) and 17q21.32 (rs72823592, P(meta) = 9.3 × 10(-9), OR[A] = 0.77). The search for syndrome-related susceptibility alleles identified significant associations for GAEs at 2q22.3 (rs10496964, P(meta) = 9.1 × 10(-9), OR[T] = 0.68) and at 1q43 for JME (rs12059546, P(meta) = 4.1 × 10(-8), OR[G] = 1.42). Suggestive evidence for an association with GGEs was found in the region 2q24.3 (rs11890028, P(meta) = 4.0 × 10(-6)) nearby the SCN1A gene, which is currently the gene with the largest number of known epilepsy-related mutations. The associated regions harbor high-ranking candidate genes: CHRM3 at 1q43, VRK2 at 2p16.1, ZEB2 at 2q22.3, SCN1A at 2q24.3 and PNPO at 17q21.32. Further replication efforts are necessary to elucidate whether these positional candidate genes contribute to the heritability of the common GGE syndromes.